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Journal of Virology, May 1999, p. 4341-4349, Vol. 73, No. 5
Department of Microbiology, Indiana
University, Bloomington, Indiana 47405,1 and
Department of Chemistry, University of Texas at Austin, Austin,
Texas 787122
Received 9 October 1998/Accepted 18 January 1999
Interactions between Rev and the Rev-responsive element (RRE)
control the order, rate, and extent of gene expression in human immunodeficiency virus type 1. Rev decoys may therefore prove to be
useful RNA therapeutics for the treatment of AIDS. To improve upon the current generation of Rev decoys that bind single Rev molecules, it would be useful to generate polyvalent Rev decoys that
could bind multiple Rev molecules. J. Kjems and P. A. Sharp (J. Virol. 67:4769-4776, 1993) originally constructed functional polyvalent Rev decoys, but the structural context of these polyvalent decoys remains unclear, and it has been argued that the individual decoys were either structurally discrete (Kjems and Sharp, J. Virol. 67:4769-4776, 1993) or were part of an extended helix (R. W. Zemmel et al., Mol. Biol. 258:763-777, 1996). To resolve the differences between these models, we have designed and synthesized concatemers of Rev-binding elements (RBEs) that fold to form
multiple, discrete, high-affinity Rev-binding sites. We find that the
concatenated RBEs can facilitate the cytoplasmic transport of
viral mRNAs and therefore likely bind multiple Rev molecules. These
artificial RREs may simultaneously sequester Rev and hinder access to
the cellular transport machinery.
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Polyvalent Rev Decoys Act as Artificial
Rev-Responsive Elements
*
Corresponding author. Mailing address: Department of
Chemistry, ICMB A4800, University of Texas at Austin, Austin, TX 78712. Phone: (512) 471-6445. Fax: (512) 471-7014. E-mail:
andy.ellington{at}mail.utexas.edu.
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